Your search keyword '"Ramasoota, Pongrama"' showing total 11 results

1. Potential Protective Effect of Dengue NS1 Human Monoclonal Antibodies against Dengue and Zika Virus Infections.

Author

Sootichote, Rochanawan, Puangmanee, Wilarat, Benjathummarak, Surachet, Kowaboot, Siriporn, Yamanaka, Atsushi, Boonnak, Korbporn, Ampawong, Sumate, Chatchen, Supawat, Ramasoota, Pongrama, and Pitaksajjakul, Pannamthip

Subjects

ZIKA virus infections, DENGUE viruses, MONOCLONAL antibodies, PLATELET-derived growth factor, MACROPHAGE inflammatory proteins

Abstract

Due to the lack of an effective therapeutic treatment to flavivirus, dengue virus (DENV) nonstructural protein 1 (NS1) has been considered to develop a vaccine owing to its lack of a role in antibody-dependent enhancement (ADE). However, both NS1 and its antibody have shown cross-reactivity to host molecules and have stimulated anti-DENV NS1 antibody-mediated endothelial damage and platelet dysfunction. To overcome the pathogenic events and reactogenicity, human monoclonal antibodies (HuMAbs) against DENV NS1 were generated from DENV-infected patients. Herein, the four DENV NS1-specific HuMAbs revealed the therapeutic effects in viral neutralization, reduction of viral replication, and enhancement of cell cytolysis of DENV and zika virus (ZIKV) via complement pathway. Furthermore, we demonstrate that DENV and ZIKV NS1 trigger endothelial dysfunction, leading to vascular permeability in vitro. Nevertheless, the pathogenic effects from NS1 were impeded by 2 HuMAbs (D25-4D4C3 and D25-2B11E7) and also protected the massive cytokines stimulation (interleukin [IL-]-1b, IL-1ra, IL-2, IL-4, IL-5, IL-6, IL-8, IL-9, IL-13, IL-17, eotaxin, granulocyte colony-stimulating factor, granulocyte-macrophage colony-stimulating factor, Inducible protein-10, monocyte chemoattractant protein-1, macrophage inflammatory protein [MIP]-1 α, MIP-1β, tumor necrosis factor-α, platelet-derived growth factor, and RANTES). Collectively, our findings suggest that the novel protective NS1 monoclonal antibodies generated from humans has multiple therapeutic benefits against DENV and ZIKV infections. [ABSTRACT FROM AUTHOR]

Published

2023

2. Chimeric flavivirus enables evaluation of antibodies against dengue virus envelope protein in vitro and in vivo.

Author

Kurosu, Takeshi, Hanabara, Keiko, Asai, Azusa, Pambudi, Sabar, Phanthanawiboon, Supranee, Omokoko, Magot Diata, Ono, Ken-ichiro, Saijo, Masayuki, Ramasoota, Pongrama, and Ikuta, Kazuyoshi

Subjects

DENGUE viruses, ANTIBODY-dependent enhancement, FLAVIVIRUSES, JAPANESE encephalitis viruses, INTERFERONS

Abstract

In a secondary dengue virus (DENV) infection, the presence of non-neutralizing antibodies (Abs), developed during a previous infection with a different DENV serotype, is thought to worsen clinical outcomes by enhancing viral production. This phenomenon is called antibody-dependent enhancement (ADE) of infection, and it has delayed the development of therapeutic Abs and vaccines against DENV, as they must be evaluated for the potential to induce ADE. Unfortunately, limited replication of DENV clinical isolates in vitro and in experimental animals hinders this evaluation process. We have, therefore, constructed a recombinant chimeric flavivirus (DV2ChimV), which carries premembrane (prM) and envelope (E) genes of type 2 DENV (DENV-2) R05-624 clinical (Thai) isolate in a backbone of Japanese encephalitis virus (Nakayama strain). DENV E-protein is the most important viral target, not only for neutralizing Abs, but also for infection-enhancing Abs. In contrast to DENV-2 R05-624, DV2ChimV replicated efficiently in cultured mammalian cells and was lethal in interferon-α/β–γ-receptor double-knockout mice. With DV2ChimV, we were able to perform neutralization assays, in vitro and in vivo ADE assays, and in vivo protection assays. These results suggest that the chimeric virus is a powerful tool for evaluation of Abs against DENV. [ABSTRACT FROM AUTHOR]

Published

2020

3. Generation and characterization of cross neutralizing human monoclonal antibody against 4 serotypes of dengue virus without enhancing activity.

Author

Injampa, Subenya, Muenngern, Nataya, Pipattanaboon, Chonlatip, Benjathummarak, Surachet, Boonha, Khwanchit, Hananantachai, Hathairad, Wongwit, Waranya, Ramasoota, Pongrama, and Pitaksajjakul, Pannamthip

Subjects

DENGUE viruses, MONOCLONAL antibodies, SEROTYPES, PLASMIDS, ANTIBODY-dependent enhancement

Abstract

Background. Dengue disease is a leading cause of illness and death in the tropics and subtropics. Most severe cases occur among patients secondarily infected with a different dengue virus (DENV) serotype compared with that from the first infection, resulting in antibody-dependent enhancement activity (ADE). Our previous study generated the neutralizing human monoclonal antibody, D23-1B3B9 (B3B9), targeting the first domain II of E protein, which showed strong neutralizing activity (NT) against all four DENV serotypes. However, at sub-neutralizing concentrations, it showed ADE activity in vitro. Methods. In this study, we constructed a new expression plasmid using the existing IgG heavy chain plasmid as a template for Fc modification at position N297Q by site-directed mutagenesis. The resulting plasmid was then co-transfected with a light chain plasmid to produce full recombinant IgG (rIgG) in mammalian cells (N297Q-B3B9). This rIgG was characterized for neutralizing and enhancing activity by using different FcR bearing cells. To produce sufficient quantities of B3B9 rIgG for further characterization, CHO-K1 cells stably secreting N297Q-B3B9 rIgG were then established. Results. The generated N297Q-B3B9 rIgG which targets the conserved N-terminal fusion loop ofDENVenvelope protein showed the same cross-neutralizing activity to all four DENV serotypes as those of wild type rIgG. In both FcRI- and RII-bearing THP- 1 cells and FcRII-bearing K562 cells, N297Q-B3B9 rIgG lacked ADE activity against all DENV serotypes at sub-neutralizing concentrations. Fortunately, the N297Q-B3B9 rIgG secreted from stable cells showed the same patterns of NT and ADE activities as those of the N297Q-B3B9 rIgG obtained from transient expression against DENV2. Thus, the CHO-K1 stably expressing N297Q-B3B9 HuMAb can be developed as high producer stable cells and used to produce sufficient amounts of antibody for further characterization as a promising dengue therapeutic candidate. Discussion. Human monoclonal antibody, targeted to fusion loop of envelope domainII (EDII), was generated and showed cross-neutralizing activity to 4 serotypes of DENV, but did not cause any viral enhancement activity in vitro. This HuMAb could be further developed as therapeutic candidates. [ABSTRACT FROM AUTHOR]

Published

2017

4. Genomic studies of envelope gene sequences from mosquito and human samples from Bangkok, Thailand.

Author

Pitaksajjakul, Pannamthip, Benjathummarak, Surachet, Son, Hyun, Thongrungkiat, Supatra, and Ramasoota, Pongrama

Subjects

GENOMICS, MOSQUITO genetics, DENGUE viruses, HOSTS (Biology), BIOLOGICAL variation

Abstract

Dengue virus (DENV) is an RNA virus showing a high degree of genetic variation as a consequence of its proofreading inability. This variation plays an important role in virus evolution and pathogenesis. Although levels of within-host genetic variation are similar following equilibrium, variation among different hosts is frequently different. To identify dengue quasispecies present among two hosts, we collected patient samples from six acute DENV cases and two pools of Aedes aegypti mosquitoes and analyzed the genetic variation of regions of the viral envelope gene. Among human and mosquito samples, we found three major clusters originating from two subpopulations. Although several shared lineages were observed in the two hosts, only one lineage showing evidence of neutral selection was observed among two hosts. Taken together, our data provide evidence for the existence of a DENV quasispecies, with less genetic variation observed in mosquitoes than humans and with circulating lineages found in both host types. [ABSTRACT FROM AUTHOR]

Published

2016

5. Low Levels of Antibody-Dependent Enhancement in Vitro Using Viruses and Plasma from Dengue Patients.

Author

Chaichana, Panjaporn, Okabayashi, Tamaki, Puiprom, Orapim, Sasayama, Mikiko, Sasaki, Tadahiro, Yamashita, Akifumi, Ramasoota, Pongrama, Kurosu, Takeshi, and Ikuta, Kazuyoshi

Subjects

DENGUE, IMMUNOGLOBULINS, BLOOD plasma, DENGUE viruses, SEROTYPES, DENGUE hemorrhagic fever, PATIENTS

Abstract

Background: The majority of dengue patients infected with any serotype of dengue virus (DENV) are asymptomatic, but the remainder may develop a wide spectrum of clinical symptoms, ranging from mild dengue fever (DF) to severe dengue hemorrhagic fever (DHF). Severe cases occur more often in patients who experience a secondary infection with a different virus serotype. A phenomenon called antibody-dependent enhancement (ADE) has been proposed to explain the onset of these severe cases, but the exact mechanism of ADE remains unclear. Methodology/Principal Finding: Virus neutralization and ADE assays were performed using ultracentrifugation supernatants of acute-phase sera from patients with secondary infections or human monoclonal antibodies (HuMAbs) as anti-DENV antibodies. Virus sources included infectious serum-derived viruses from the ultracentrifugation precipitates, laboratory-culture adapted DENV, or recombinant DENVs derived from patient sera. In contrast to the high levels of ADE observed with laboratory virus strains, low ADE was observed with autologous patient-derived viruses, when patient sera were used to provide the antibody component in the ADE assays. Similar results were obtained using samples from DF and DHF patients. Recombinant-viruses derived from DHF patients showed only minor differences in neutralization and ADE activity in the presence of HuMAbs or plasma derived from the same DHF patient. Conclusion/Significance: Serum or plasma taken from patients during the acute phase of a secondary infection showed high levels of ADE, but no neutralization activity, when assayed in the presence of laboratory-adapted virus strains. By contrast, serum or plasma from the same patient showed high levels of neutralization activity but failed to induce significant ADE when the assays were performed with autologous virus. These results demonstrate the significance of the virus source when measuring ADE. They also suggest that repeated passage of DENV in cell culture has endowed it with the capacity to induce high levels of ADE. [ABSTRACT FROM AUTHOR]

Published

2014

6. Cross-reactivity of human monoclonal antibodies generated with peripheral blood lymphocytes from dengue patients with Japanese encephalitis virus.

Author

Pipattanaboon, Chonlatip, Sasaki, Tadahiro, Nishimura, Mitsuhiro, Setthapramote, Chayanee, Pitaksajjakul, Pannamthip, Leaungwutiwong, Pornsawan, Limkittikul, Kriengsak, Puiprom, Orapim, Sasayama, Mikiko, Chaichana, Panjaporn, Okabayashi, Tamaki, Kurosu, Takeshi, Ono, Ken-ichiro, Ramasoota, Pongrama, and Ikuta, Kazuyoshi

Subjects

HYBRIDOMAS, IMMUNOGLOBULINS, JAPANESE encephalitis viruses, DENGUE viruses, LYMPHOCYTES, DENGUE, PATIENTS

Abstract

Background: Hybridomas that produce human monoclonal antibodies (HuMAbs) against Dengue virus (DV) had been prepared previously using peripheral blood lymphocytes from patients with DV during the acute and convalescent phases of a secondary infection. Anti-DV envelope glycoprotein (E) 99 clones, anti-DV premembrane protein (prM) 8 clones, and anti-DV nonstructural protein 1 (NS1) 4 clones were derived from four acute-phase patients, and anti-DV E 2 clones, anti-DV prM 2 clones, and anti-DV NS1 8 clones were derived from five convalescent-phase patients. Methods and results: In the present study, we examined whether these clones cross-reacted with Japanese encephalitis virus (JEV), which belongs to the same virus family. Forty-six of the above-described 99 (46/99) anti-E, 0/8 anti-prM, and 2/4 anti-NS1 HuMAbs from acute-phase, and 0/2 anti-E, 0/2 anti-prM, and 5/8 anti-NS1 HuMAbs from convalescent-phase showed neutralizing activity against JEV. Thus, most of the anti-E and anti-NS1 (but not the anti-prM) antibodies cross-reacted with JEV and neutralized this virus. Interestingly, 3/46 anti-E HuMAbs derived from acute-phase patients and 3/5 anti-NS1 HuMAbs from convalescent-phase patients showed particularly high neutralizing activity against JEV. Consequently, the HuMAbs showing neutralization against JEV mostly consisted of two populations: one was HuMAbs recognizing DV E and showing neutralization activity against all four DV serotypes (complex-type) and the other was HuMAbs recognizing DV NS1 and showing subcomplex-type cross-reaction with DV. Conclusion: Anti-DV E from acute phase (46/99) and anti-DV NS1 (7/12) indicate neutralizing activity against JEV. In particular, three of 46 anti-DV E clones from acute phase and three of five anti-NS1 clones from convalescent phase showed strong neutralizing activity against JEV. [ABSTRACT FROM AUTHOR]

Published

2013

7. Limited cross-reactivity of mouse monoclonal antibodies against Dengue virus capsid protein among four serotypes.

Author

Noda, Megumi, Masrinoul, Promsin, Punkum, Chaweewan, Pipattanaboon, Chonlatip, Ramasoota, Pongrama, Setthapramote, Chayanee, Sasaki, Tadahiro, Sasayama, Mikiko, Yamashita, Akifumi, Kurosu, Takeshi, Ikuta, Kazuyoshi, and Okabayashi, Tamaki

Subjects

MONOCLONAL antibodies, DENGUE viruses, CAPSIDS, AMINO acid sequence, JAPANESE encephalitis viruses, SEROTYPES

Abstract

Background: Dengue illness is one of the important mosquito-borne viral diseases in tropical and subtropical regions. Four serotypes of dengue virus (DENV-1, DENV-2, DENV-3, and DENV-4) are classified in the Flavivirus genus of the family Flaviviridae. We prepared monoclonal antibodies against DENV capsid protein from mice immunized with DENV-2 and determined the cross-reactivity with each serotype of DENV and Japanese encephalitis virus. Methods and results: To clarify the relationship between the cross-reactivity of monoclonal antibodies and the diversity of these viruses, we examined the situations of flaviviruses by analyses of phylogenetic trees. Among a total of 60 prepared monoclonal antibodies specific for DENV, five monoclonal antibodies stained the nuclei of infected cells and were found to be specific to the capsid protein. Three were specific to DENV-2, while the other two were cross-reactive with DENV-2 and DENV-4. No monoclonal antibodies were cross-reactive with all four serotypes. Phylogenetic analysis of DENV amino acid sequences of the capsid protein revealed that DENV-2 and DENV-4 were clustered in the same branch, while DENV-1 and DENV-3 were clustered in the other branch. However, these classifications of the capsid protein were different from those of the envelope and nonstructural 1 proteins. Phylogenetic distances between the four serotypes of DENV were as different as those of other flaviviruses, such as Japanese encephalitis virus and West Nile virus. Large variations in the DENV serotypes were comparable with the differences between species of flavivirus. Furthermore, the diversity of flavivirus capsid protein was much greater than that of envelope and nonstructural 1 proteins. Conclusion: In this study, we produced specific monoclonal antibodies that can be used to detect DENV-2 capsid protein, but not a cross-reactive one with all serotypes of DENV capsid protein. The high diversity of the DENV capsid protein sequence by phylogenetic analysis supported the low cross-reactivity of monoclonal antibodies against DENV capsid protein. [ABSTRACT FROM AUTHOR]

Published

2012

8. A replication competent luciferase-secreting DENV2 reporter for sero-epidemiological surveillance of neutralizing and enhancing antibodies.

Author

Saipin, Krongkan, Thaisomboonsuk, Butsaya, Siridechadilok, Bunpote, Chaitaveep, Nithinart, Ramasoota, Pongrama, Puttikhunt, Chunya, Sangiambut, Sutha, Jones, Anthony, Kraivong, Romchat, Sriburi, Rungtawan, Keelapang, Poonsook, Sittisombut, Nopporn, and Junjhon, Jiraphan

Subjects

*IMMUNOGLOBULINS, *DENGUE viruses, *MONOCLONAL antibodies, *LUCIFERASES, *CELL lines, *PREVENTIVE medicine, *FLAVIVIRUSES

Abstract

Dengue virus (DENV) specific neutralizing and enhancing antibodies play crucial roles in dengue disease prevention and pathogenesis. DENV reporters are gaining popularity in the evaluation of these antibodies; their accessibility and acceptance may improve with more efficient production systems and indications of their antigenic equivalence to the wild-type virus. This study aimed to generate a replication competent luciferase-secreting DENV reporter (LucDENV2) and evaluate its feasibility in neutralizing and infection-enhancing antibody assays in comparison with wild-type DENV2, strain 16681, and a luciferase-secreting, single-round infectious DENV2 reporter (LucSIP). LucDENV2 replicated to similarly high levels as that of the parent 16681 virus in a commonly used mosquito cell line. LucDENV2 was neutralized in an antibody concentration-dependent manner by a monoclonal antibody specific to the flavivirus fusion loop and two antibodies specific to the E domain III, which closely resembled the neutralization patterns employing the LucSIP and wild-type DENV2. Parallel analysis of LucDENV2 and wild-type DENV2 revealed good agreement between the luciferase-based and focus-based neutralization and enhancement assays in a 96-well microplate format when employed against a set of clinical sera, suggesting comparable antigenic properties of LucDENV2 with those of the parent virus. The high-titer, replication competent, luciferase-secreting DENV reporter presented here should be a useful tool for fast and reliable quantitation of neutralizing and infection-enhancing antibodies in populations living in DENV-endemic areas. • High-titer, replication competent LucDENV2 generated in widely used mosquito cells. • LucDENV2, LucSIP and wild-type DENV2 similarly neutralized by anti-E antibodies. • Feasibility of LucDENV2 used in LRNT assay was shown with 30 DENV2 clinical sera. • Comparable antibody-mediated infection-enhancement of LucDENV2 and wild-type DENV2. [ABSTRACT FROM AUTHOR]

Published

2022

9. Antibody germline characterization of cross-neutralizing human IgGs against 4 serotypes of dengue virus.

Author

Pitaksajjakul, Pannamthip, Benjathummarak, Surachet, Pipattanaboon, Chonlatip, Wongwit, Waranya, Okabayashi, Tamaki, Kuhara, Motoki, Misaki, Ryo, Fujiyama, Kazuhito, and Ramasoota, Pongrama

Subjects

*GERM cells, *DENGUE viruses, *IMMUNOGLOBULIN G, *SEROTYPES, *EMBRYOLOGY

Abstract

Highlights: [•] VH and VL were isolated from cross-neutralizing 19 HuMAbs specific to dengue virus. [•] VH and VL were analysed with germline sequences using IMGT database. [•] 10 VH and 10 VL germlines were used by our 19 HuMAbs. [•] VH and VL of 3 HuMAbs were used to produce human IgG. [ABSTRACT FROM AUTHOR]

Published

2014

10. Dengue virus neutralization and antibody-dependent enhancement activities of human monoclonal antibodies derived from dengue patients at acute phase of secondary infection.

Author

Sasaki, Tadahiro, Setthapramote, Chayanee, Kurosu, Takeshi, Nishimura, Mitsuhiro, Asai, Azusa, Omokoko, Magot D., Pipattanaboon, Chonlatip, Pitaksajjakul, Pannamthip, Limkittikul, Kriengsak, Subchareon, Arunee, Chaichana, Panjaporn, Okabayashi, Tamaki, Hirai, Itaru, Leaungwutiwong, Pornsawan, Misaki, Ryo, Fujiyama, Kazuhito, Ono, Ken-ichiro, Okuno, Yoshinobu, Ramasoota, Pongrama, and Ikuta, Kazuyoshi

Subjects

*DENGUE viruses, *IMMUNOGLOBULINS, *ENZYME activation, *MONOCLONAL antibodies, *DENGUE, *VIRUS-induced enzymes, *PATIENTS

Abstract

Highlights: [•] Severe cases are often observed in patients of 2nd infection with dengue virus. [•] ADE is the hypothesis to explain the mechanism for severe cases 2nd infection. [•] Human monoclonal antibodies to neutralize 1–4 serotypes were prepared. [•] No difference was observed in ADE activities between antibodies from DF and DHF. [Copyright &y& Elsevier]

Published

2013

11. Human monoclonal antibodies to neutralize all dengue virus serotypes using lymphocytes from patients at acute phase of the secondary infection

Author

Setthapramote, Chayanee, Sasaki, Tadahiro, Puiprom, Orapim, Limkittikul, Kriengsak, Pitaksajjakul, Pannamthip, Pipattanaboon, Chonlatip, Sasayama, Mikiko, Leuangwutiwong, Pornsawan, Phumratanaprapin, Weerapong, Chamnachanan, Supat, Kusolsuk, Teera, Jittmittraphap, Akanitt, Asai, Azusa, Arias, Juan Fernando, Hirai, Itaru, Kuhara, Motoki, Okuno, Yoshinobu, Kurosu, Takeshi, Ramasoota, Pongrama, and Ikuta, Kazuyoshi

Subjects

*MONOCLONAL antibodies, *NEUTRALIZATION (Chemistry), *DENGUE viruses, *LYMPHOCYTES, *VIRUS diseases, *SEROTYPES, *PUBLIC health

Abstract

Abstract: The global spread of the four dengue virus serotypes (DENV-1 to -4) has made this virus a major and growing public health concern. Generally, pre-existing neutralizing antibodies derived from primary infection play a significant role in protecting against subsequent infection with the same serotype. By contrast, these pre-existing antibodies are believed to mediate a non-protective response to subsequent heterotypic DENV infections, leading to the onset of dengue illness. In this study, we prepared hybridomas producing human monoclonal antibodies (HuMAbs) against DENV using peripheral blood mononuclear cells (PBMCs) from patients in the acute phase (around 1week after the onset of illness) or the convalescent phase (around 2weeks after the onset of illness) of secondary infection. Interestingly, a larger number of hybridoma clones was obtained from patients in the acute phase than from those in the convalescent phase. Most HuMAbs from acute-phase infections were cross-reactive with all four DENV serotypes and showed significant neutralization activity to all four DENV serotypes. Thus, secondary DENV infection plays a significant role in stimulating memory cells to transiently increase the number of antibody-secreting plasma cells in patients in the early phase after the secondary infection. These HuMAbs will enable us to better understand the protective and pathogenic effects of DENV infection, which could vary greatly among secondarily-infected individuals. [Copyright &y& Elsevier]

Published

2012